Your search keyword '"Fenghua Yuan"' showing total 90 results

1. Fanconi anemia associated protein 20 (FAAP20) plays an essential role in homology-directed repair of DNA double-strand breaks

Author

Anna Palovcak, Fenghua Yuan, Ramiro Verdun, Liang Luo, and Yanbin Zhang

Subjects

Biology (General), QH301-705.5

Abstract

Abstract FAAP20 is a Fanconi anemia (FA) protein that associates with the FA core complex to promote FANCD2/FANCI monoubiquitination and activate the damage response to interstrand crosslink damage. Here, we report that FAAP20 has a marked role in homologous recombination at a DNA double-strand break not associated with an ICL and separable from its binding partner FANCA. While FAAP20’s role in homologous recombination is not dependent on FANCA, we found that FAAP20 stimulates FANCA’s biochemical activity in vitro and participates in the single-strand annealing pathway of double-strand break repair in a FANCA-dependent manner. This indicates that FAAP20 has roles in several homology-directed repair pathways. Like other homology-directed repair factors, FAAP20 loss causes a reduction in nuclear RAD51 Irradiation-induced foci; and sensitizes cancer cells to ionizing radiation and PARP inhibition. In summary, FAAP20 participates in DNA double strand break repair by supporting homologous recombination in a non-redundant manner to FANCA, and single-strand annealing repair via FANCA-mediated strand annealing activity.

Published

2023

2. A convenient polyculture system that controls a shrimp viral disease with a high transmission rate

Author

Muhua Wang, Yonggui Chen, Zhong Zhao, Shaoping Weng, Jinchuan Yang, Shangyun Liu, Chang Liu, Fenghua Yuan, Bin Ai, Haiqing Zhang, Mingyan Zhang, Lirong Lu, Kai Yuan, Zhaolong Yu, Bibo Mo, Xinjian Liu, Chunlei Gai, Yijun Li, Renjie Lu, Zhiwei Zhong, Luwei Zheng, Guocan Feng, Shengwen Calvin Li, and Jianguo He

Subjects

Biology (General), QH301-705.5

Abstract

Wang et al. develop a shrimp polyculture system that prevents white spot syndrome outbreaks by introducing specific fish species. The system is easy to implement and requires no special biosecurity measures which makes it ideal for small-scale farmers.

Published

2021

3. Fanconi anemia pathway as a prospective target for cancer intervention

Author

Wenjun Liu, Anna Palovcak, Fang Li, Alyan Zafar, Fenghua Yuan, and Yanbin Zhang

Subjects

Fanconi anemia, DNA repair, Tumorigenesis, Cancer intervention, Biotechnology, TP248.13-248.65, Biology (General), QH301-705.5, Biochemistry, QD415-436

Abstract

Abstract Fanconi anemia (FA) is a recessive genetic disorder caused by biallelic mutations in at least one of 22 FA genes. Beyond its pathological presentation of bone marrow failure and congenital abnormalities, FA is associated with chromosomal abnormality and genomic instability, and thus represents a genetic vulnerability for cancer predisposition. The cancer relevance of the FA pathway is further established with the pervasive occurrence of FA gene alterations in somatic cancers and observations of FA pathway activation-associated chemotherapy resistance. In this article we describe the role of the FA pathway in canonical interstrand crosslink (ICL) repair and possible contributions of FA gene alterations to cancer development. We also discuss the perspectives and potential of targeting the FA pathway for cancer intervention.

Published

2020

4. The Applications of Nanopore Sequencing Technology in Pathogenic Microorganism Detection

Author

Xiaojian Zhu, Shanshan Yan, Fenghua Yuan, and Shaogui Wan

Subjects

Infectious and parasitic diseases, RC109-216, Microbiology, QR1-502

Abstract

Infectious diseases are major threats to human health and lead to a serious public health burden. The emergence of new pathogens and the mutation of known pathogens challenge our ability to diagnose and control infectious diseases. Nanopore sequencing technology exhibited versatile applications in pathogenic microorganism detection due to its flexible data throughput. This review article introduced the applications of nanopore sequencing in clinical microbiology and infectious diseases management, including the monitoring of emerging infectious diseases outbreak, identification of pathogen drug resistance, and disease-related microbial communities characterization.

Published

2020

5. Stitching up broken DNA ends by FANCA

Author

Anna Palovcak, Wenjun Liu, Fenghua Yuan, and Yanbin Zhang

Subjects

fanca, fanconi anemia, double strand break repair, interstrand crosslink repair, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

RAD52 rejoins resected broken DNA ends by mediating single-strand annealing. Our recent work elucidates that FANCA, a Fanconi anemia protein, also directly repairs double-strand breaks (DSBs) by catalyzing annealing of single-stranded DNA. FANCA and RAD52 likely play complementary roles to each other to prevent deleterious consequences of DSBs. Abbreviations: DSBs: DNA double-strand breaks; ICL: interstrand crosslink; ssDNA: single-stranded DNA; HR: homologous recombination; SSA: single-strand annealing; MMEJ: microhomology-mediated end joining; NHEJ: non-homologous end joining; GFP: green fluorescence protein

Published

2018

6. Human Fanconi anemia complementation group a protein stimulates the 5' flap endonuclease activity of FEN1.

Author

Liangyue Qian, Fenghua Yuan, Paola Rodriguez-Tello, Suyog Padgaonkar, and Yanbin Zhang

Subjects

Medicine, Science

Abstract

In eukaryotic cells, Flap endonuclease 1 (FEN1) is a major structure-specific endonuclease that processes 5' flapped structures during maturation of lagging strand DNA synthesis, long patch base excision repair, and rescue of stalled replication forks. Here we report that fanconi anemia complementation group A protein (FANCA), a protein that recognizes 5' flap structures and is involved in DNA repair and maintenance of replication forks, constantly stimulates FEN1-mediated incision of both DNA and RNA flaps. Kinetic analyses indicate that FANCA stimulates FEN1 by increasing the turnover rate of FEN1 and altering its substrate affinity. More importantly, six pathogenic FANCA mutants are significantly less efficient than the wild-type at stimulating FEN1 endonuclease activity, implicating that regulation of FEN1 by FANCA contributes to the maintenance of genomic stability.

Published

2013

7. A Lightweight Sensor Network Management System Design.

Author

Fenghua Yuan, Wen-Zhan Song 0001, Nina M. Peterson, Yang Peng, Lei Wang, Behrooz A. Shirazi, and Richard LaHusen

Published

2008

8. A network-flow approach to timing-driven incremental placement for ASICs.

Author

Shantanu Dutt, Huan Ren, Fenghua Yuan, and Vishal Suthar

Published

2006

9. Time-Optimum Packet Scheduling for Many-to-One Routing in Wireless Sensor Networks.

Author

Wen-Zhan Song 0001, Fenghua Yuan, and Richard LaHusen

Published

2006

10. Abstract 3983: Defining the role of FANCA in breast cancer development and cell cycle progression

Author

Liang Luo, Wenjun Liu, Anna Palovcak, Fenghua Yuan, Fang Li, Daniel Calkins, Yan Li, Karoline Briegel, Daniel Bilbao, Evan Roberts, Christian Mason, Zhao-Jun Liu, Sylvia Daunert, and Yanbin Zhang

Subjects

Cancer Research, Oncology

Abstract

FANCA is one of the 22 known Fanconi anemia (FA) pathway genes and is indispensable for interstrand crosslink (ICL) repair. It is reported that FANCA is responsible for about 64% of FA cases and one important clinical characterization of FA patients is predisposition to cancer. However, analysis of TCGA database reveals that FANCA level is elevated in breast cancer patients, especially in ER- breast cancer, which is associated with the methylation status at the S-shore of CpG island ahead of FANCA gene. Moreover, the FANCA level is negatively correlated with the survival rate of breast cancer patients. To understand the implication of FANCA in breast cancer development, we have targeted FANCA by either CRISPR mediated knock-out (KO) or shRNA mediated knockdown (KD) in MDA-MB-231 breast cancer cells. Our data suggest that depletion of FANCA protein inhibits breast cancer growth both in vitro and in vivo. On the other hand, overexpressing FANCA in low-FANCA breast cancer cell line MDA-MB-468 promotes cancer cell proliferation. Cell cycle profiling reveals an inefficiency of MDA-MB-231 FANCA KO cells in G1 to S transition due to p21 and p27 upregulation in FANCA KO cells. In addition, the proliferation inefficiency in MDA-MB-231 FANCA KO cells is caused by Rb hypophosphorylation. Therefore, we conclude that FANCA contributes to the breast cancer development by promoting cell cycle progression through Rb/E2F signaling pathway. Our immunoprecipitation (IP) results indicate that in MDA-MB-231, FANCA is interacting with HES1, which is a transcription suppressor that binds to the promoter region of CDKN1A and CDKN1B to promote cell cycle progression, explaining how FANCA participates in cell cycle progression in breast cancer. Citation Format: Liang Luo, Wenjun Liu, Anna Palovcak, Fenghua Yuan, Fang Li, Daniel Calkins, Yan Li, Karoline Briegel, Daniel Bilbao, Evan Roberts, Christian Mason, Zhao-Jun Liu, Sylvia Daunert, Yanbin Zhang. Defining the role of FANCA in breast cancer development and cell cycle progression. [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2023; Part 1 (Regular and Invited Abstracts); 2023 Apr 14-19; Orlando, FL. Philadelphia (PA): AACR; Cancer Res 2023;83(7_Suppl):Abstract nr 3983.

Published

2023

11. Time-optimum packet scheduling for many-to-one routing in wireless sensor networks.

Author

Wen-Zhan Song 0001, Fenghua Yuan, Richard LaHusen, and Behrooz A. Shirazi

Published

2007

12. Sub-pixel position estimation algorithm based on Gaussian fitting and sampling theorem interpolation for wafer alignment

Author

Jinghao Xu, Yang Bu, Ting Shu, Lili Fan, Shaoqing Wang, Fenghua Yuan, Songyong Pan, Xiangzhao Wang, Fengzhao Dai, and Xiaona Yan

Subjects

Pixel, Computer science, Gaussian, Noise reduction, Image processing, Atomic and Molecular Physics, and Optics, Edge detection, symbols.namesake, Robustness (computer science), symbols, Nyquist–Shannon sampling theorem, Electrical and Electronic Engineering, Engineering (miscellaneous), Algorithm, Interpolation

Abstract

Wafer alignment is the core technique of lithographic tools. Image-processing-based wafer alignment techniques are commonly used in lithographic tools. An alignment algorithm is used to analyze the alignment mark image for obtaining the mark position. The accuracy and speed of the alignment algorithm are very important for guaranteeing the overlay and throughput of lithographic tools. The most commonly used algorithm in image-processing-based alignment techniques is the self-correlation method. This method has a high accuracy, but the calculation is complex, and the calculation speed is slow. In this paper, we propose a sub-pixel position estimation algorithm based on Gaussian fitting and sampling theorem interpolation. The algorithm first reconstructs the alignment signal by sampling theorem interpolation and then obtains the sub-pixel position of the mark by Gaussian fitting. The accuracy and robustness of the algorithm are verified by testing the simulated marks and experimentally captured marks. The repeat accuracy can reach 1/100 pixels, which is in the same level with the self-correlation method. The calculation speed is highly improved compared with the self-correlation method, which needs only about 1/3 of even short calculation time.

Published

2021

13. Effect of Reinforcement Corrosion Sediment Distribution Characteristics on Concrete Damage Behavior

Author

Fenghua Yuan, Qing Zhang, and Xiaozhou Xia

Subjects

Biomaterials, Distribution (number theory), Mechanics of Materials, Modeling and Simulation, Environmental science, Sediment, Reinforcement corrosion, Geotechnical engineering, Electrical and Electronic Engineering, Computer Science Applications

Published

2019

14. Fanconi anemia pathway as a prospective target for cancer intervention

Author

Fang Li, Fenghua Yuan, Yanbin Zhang, Wenjun Liu, Alyan Zafar, and Anna Palovcak

Subjects

Genome instability, DNA repair, lcsh:Biotechnology, Review, medicine.disease_cause, General Biochemistry, Genetics and Molecular Biology, lcsh:Biochemistry, 03 medical and health sciences, 0302 clinical medicine, Fanconi anemia, lcsh:TP248.13-248.65, medicine, lcsh:QD415-436, lcsh:QH301-705.5, Gene, 030304 developmental biology, 0303 health sciences, business.industry, Genetic disorder, Bone marrow failure, Cancer, Cancer intervention, medicine.disease, 3. Good health, lcsh:Biology (General), 030220 oncology & carcinogenesis, Tumorigenesis, Cancer research, business, Carcinogenesis

Abstract

Fanconi anemia (FA) is a recessive genetic disorder caused by biallelic mutations in at least one of 22 FA genes. Beyond its pathological presentation of bone marrow failure and congenital abnormalities, FA is associated with chromosomal abnormality and genomic instability, and thus represents a genetic vulnerability for cancer predisposition. The cancer relevance of the FA pathway is further established with the pervasive occurrence of FA gene alterations in somatic cancers and observations of FA pathway activation-associated chemotherapy resistance. In this article we describe the role of the FA pathway in canonical interstrand crosslink (ICL) repair and possible contributions of FA gene alterations to cancer development. We also discuss the perspectives and potential of targeting the FA pathway for cancer intervention.

Published

2020

15. Reconstitution of 5'-directed human mismatch repair in a purified system

Author

Yanbin Zhang, Fenghua Yuan, Presnell, Steven R., Guo-Min Li, Tian, Keli, Gu, Liya, Gao, Yin, and Tomkinson, Alan E.

Subjects

DNA replication -- Research, DNA repair -- Research, Cell research, Biological sciences

Abstract

Reconstitution of 5'nick-directed mismatch repair using purified human proteins is reported. The data suggest a model for human mismatch repair involving coordinated initiation and termination of mismatch-provoked excision.

Published

2005

16. The Polycomb protein RING1B enables estrogen-mediated gene expression by promoting enhancer–promoter interaction and R-loop formation

Author

Kyutae D. Lee, Simone Sidoli, Yanbin Zhang, Lluis Morey, Liliana Garcia-Martinez, Tong Liu, Yusheng Zhang, Ramiro E. Verdun, Zheng Wang, Stephanie Stransky, and Fenghua Yuan

Subjects

Polycomb Repressive Complex 1, Transcriptional Activation, Regulation of gene expression, Estradiol, biology, AcademicSubjects/SCI00010, Gene regulation, Chromatin and Epigenetics, Estrogen Receptor alpha, RNA, RNA polymerase II, Chromatin, Cell Line, Cell biology, Enhancer Elements, Genetic, Transcription (biology), Gene expression, Genetics, biology.protein, Humans, R-Loop Structures, Promoter Regions, Genetic, Enhancer, Estrogen receptor alpha

Abstract

Polycomb complexes have traditionally been prescribed roles as transcriptional repressors, though increasing evidence demonstrate they can also activate gene expression. However, the mechanisms underlying positive gene regulation mediated by Polycomb proteins are poorly understood. Here, we show that RING1B, a core component of Polycomb Repressive Complex 1, regulates enhancer–promoter interaction of the bona fide estrogen-activated GREB1 gene. Systematic characterization of RNA:DNA hybrid formation (R-loops), nascent transcription and RNA Pol II activity upon estrogen administration revealed a key role of RING1B in gene activation by regulating R-loop formation and RNA Pol II elongation. We also found that the estrogen receptor alpha (ERα) and RNA are both necessary for full RING1B recruitment to estrogen-activated genes. Notably, RING1B recruitment was mostly unaffected upon RNA Pol II depletion. Our findings delineate the functional interplay between RING1B, RNA and ERα to safeguard chromatin architecture perturbations required for estrogen-mediated gene regulation and highlight the crosstalk between steroid hormones and Polycomb proteins to regulate oncogenic programs.

Published

2021

17. Identification of KANSARL as the first cancer predisposition fusion gene specific to the population of European ancestry origin

Author

Shunbin Ning, Jeff X. Zhou, Fenghua Yuan, Yanbin Zhang, David D. Zhuo, Ling Wang, Kesheng Wang, Liren Tang, Fengli Li, Degen Zhuo, and Xiaoyan Yang

Subjects

0301 basic medicine, Genetics, education.field_of_study, European ancestry origin, Population, Cancer, RNA-Seq, Biology, medicine.disease, Fusion gene, 03 medical and health sciences, Prostate cancer, 030104 developmental biology, The Hallmarks of Cancer, Breast cancer, Oncology, fusion gene, KANSARL, medicine, 1000 Genomes Project, RNA-seq, education, Research Paper

Abstract

// Jeff Xiwu Zhou 1, * , Xiaoyan Yang 2, * , Shunbin Ning 3, * , Ling Wang 3 , Kesheng Wang 4 , Yanbin Zhang 5 , Fenghua Yuan 5 , Fengli Li 1 , David D. Zhuo 2 , Liren Tang 2 and Degen Zhuo 2 1 Department of Medicine, School of Medicine, Ningbo University, Ningbo, China 2 SplicingCodes.com, Biotailor Inc., Palmetto Bay, FL, USA 3 Department of Internal Medicine, Quillen College of Medicine, East Tennessee State University, Johnson City, TN, USA 4 Department of Biostatistics and Epidemiology, East Tennessee State University, Johnson City, TN, USA 5 Department of Biochemistry and Molecular Biology, University of Miami, Miami, FL, USA * These authors have contributed equally to this work Correspondence to: Degen Zhuo, email: dzhuo@splicingcodes.com Keywords: KANSARL , fusion gene, European ancestry origin, RNA-seq Received: August 15, 2016 Accepted: February 20, 2017 Published: March 24, 2017 ABSTRACT Gene fusion is one of the hallmarks of cancer. Recent advances in RNA-seq of cancer transcriptomes have facilitated the discovery of fusion transcripts. In this study, we report identification of a surprisingly large number of fusion transcripts, including six KANSARL ( KANSL1 - ARL17A ) transcripts that resulted from the fusion between the KANSL1 and ARL17A genes using a RNA splicingcode model. Five of these six KANSARL fusion transcripts are novel. By systematic analysis of RNA-seq data of glioblastoma, prostate cancer, lung cancer, breast cancer, and lymphoma from different regions of the World, we have found that KANSARL fusion transcripts were rarely detected in the tumors of individuals from Asia or Africa. In contrast, they exist in 30 - 52% of the tumors from North Americans cancer patients. Analysis of CEPH/Utah Pedigree 1463 has revealed that KANSARL is a familially-inherited fusion gene. Further analysis of RNA-seq datasets of the 1000 Genome Project has indicated that KANSARL fusion gene is specific to 28.9% of the population of European ancestry origin. In summary, we demonstrated that KANSARL is the first cancer predisposition fusion gene associated with genetic backgrounds of European ancestry origin.

Published

2017

18. Measurement algorithm for wafer alignment based on principal component analysis

Author

Jinghao Xu, Xiangzhao Wang, Fengzhao Dai, Lili Fan, Shaoqing Wang, Songyong Pan, Fenghua Yuan, Ting Shu, and Yang Bu

Subjects

Image quality, Computer science, Feature extraction, Image registration, Image processing, 01 natural sciences, Atomic and Molecular Physics, and Optics, Edge detection, 010309 optics, Computer Science::Computer Vision and Pattern Recognition, 0103 physical sciences, Principal component analysis, Waveform, Electrical and Electronic Engineering, Projection (set theory), Engineering (miscellaneous), Algorithm, Computer Science::Databases

Abstract

We propose a novel measurement algorithm for wafer alignment technology based on principal component analysis (PCA) of a mark image. The waveform of the mark is extracted from the enlarged mark image, which is collected by CCD. The position of the mark center on the CCD can be calculated based on the extracted waveform. By applying PCA to the mark image, the first principal component containing position information of the mark can be obtained. Therefore PCA can be used to extract the waveform from the mark image. Compared with the typical waveform extraction method (the summed projection (SP) method), the proposed PCA method can use the position information contained in the mark image more effectively. Through simulation and experiment, it is proved that the proposed PCA method can improve the contrast of the normalized waveform, and then improve the alignment accuracy.

Published

2021

19. Histone Deacetylase 10 Regulates DNA Mismatch Repair and May Involve the Deacetylation of MutS Homolog 2

Author

Xiaohong Zhang, Rangasudhagar Radhakrishnan, Shengyan Xiang, Zhigang Yuan, Elphine Telles, David Shibata, Domenico Coppola, William S. Lane, Edward Seto, Fenghua Yuan, Yanbin Zhang, Yixuan Li, and Jia Fang

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, DNA and Chromosomes, DNA Mismatch Repair, Biochemistry, Histone Deacetylases, Histone H2A, Humans, Histone code, neoplasms, Molecular Biology, MutS Homolog 2 Protein, Histone deacetylase 5, biology, Histone deacetylase 2, nutritional and metabolic diseases, Acetylation, DNA, Cell Biology, Histone acetyltransferase, Molecular biology, digestive system diseases, MSH3, biology.protein, Histone deacetylase, HeLa Cells

Abstract

MutS homolog 2 (MSH2) is an essential DNA mismatch repair (MMR) protein. It interacts with MSH6 or MSH3 to form the MutSα or MutSβ complex, respectively, which recognize base-base mispairs and insertions/deletions and initiate the repair process. Mutation or dysregulation of MSH2 causes genomic instability that can lead to cancer. MSH2 is acetylated at its C terminus, and histone deacetylase (HDAC6) deacetylates MSH2. However, whether other regions of MSH2 can be acetylated and whether other histone deacetylases (HDACs) and histone acetyltransferases (HATs) are involved in MSH2 deacetylation/acetylation is unknown. Here, we report that MSH2 can be acetylated at Lys-73 near the N terminus. Lys-73 is highly conserved across many species. Although several Class I and II HDACs interact with MSH2, HDAC10 is the major enzyme that deacetylates MSH2 at Lys-73. Histone acetyltransferase HBO1 might acetylate this residue. HDAC10 overexpression in HeLa cells stimulates cellular DNA MMR activity, whereas HDAC10 knockdown decreases DNA MMR activity. Thus, our study identifies an HDAC10-mediated regulatory mechanism controlling the DNA mismatch repair function of MSH2.

Published

2015

20. Human DNA Exonuclease TREX1 Is Also an Exoribonuclease That Acts on Single-stranded RNA

Author

Ling Wang, Anaid Benitez, Tanmay Dutta, Murray P. Deutscher, Liya Gu, Liangyue Qian, Shunbin Ning, Lei Song, Fenghua Yuan, Yanbin Zhang, and Arun Malhotra

Subjects

Protein Conformation, RNase P, Molecular Sequence Data, RNA-dependent RNA polymerase, DNA Exonuclease, Biology, Biochemistry, Exonuclease 1, Exoribonuclease, Humans, Amino Acid Sequence, RNase H, Molecular Biology, Binding Sites, Sequence Homology, Amino Acid, RNA, DNA, Cell Biology, Phosphoproteins, Non-coding RNA, Kinetics, Exodeoxyribonucleases, Exoribonucleases, Mutation, biology.protein, Protein Multimerization

Abstract

3′ repair exonuclease 1 (TREX1) is a known DNA exonuclease involved in autoimmune disorders and the antiviral response. In this work, we show that TREX1 is also a RNA exonuclease. Purified TREX1 displays robust exoribonuclease activity that degrades single-stranded, but not double-stranded, RNA. TREX1-D200N, an Aicardi-Goutieres syndrome disease-causing mutant, is defective in degrading RNA. TREX1 activity is strongly inhibited by a stretch of pyrimidine residues as is a bacterial homolog, RNase T. Kinetic measurements indicate that the apparent Km of TREX1 for RNA is higher than that for DNA. Like RNase T, human TREX1 is active in degrading native tRNA substrates. Previously reported TREX1 crystal structures have revealed that the substrate binding sites are open enough to accommodate the extra hydroxyl group in RNA, further supporting our conclusion that TREX1 acts on RNA. These findings indicate that its RNase activity needs to be taken into account when evaluating the physiological role of TREX1. Background: 3′ repair exonuclease 1 (TREX1) is a DNase involved in autoimmune disorders and the antiviral response. Results: TREX1 also degrades single-stranded RNA or RNA in a RNA/DNA hybrid molecule. Conclusion: TREX1 is a human homolog of Escherichia coli RNase T. Significance: The novel RNase activity of TREX1 is crucial for understanding its physiological role.

Published

2015

21. Maintenance of genome stability by Fanconi anemia proteins

Author

Anna Palovcak, Yanbin Zhang, Wenjun Liu, and Fenghua Yuan

Subjects

0301 basic medicine, Genetics, Genome instability, DNA damage, DNA repair, Cancer, Review, Biology, DNA damage response, medicine.disease, Genome, General Biochemistry, Genetics and Molecular Biology, FANCA, 3. Good health, 03 medical and health sciences, 030104 developmental biology, Fanconi anemia, hemic and lymphatic diseases, medicine, Gene

Abstract

Persistent dysregulation of the DNA damage response and repair in cells causes genomic instability. The resulting genetic changes permit alterations in growth and proliferation observed in virtually all cancers. However, an unstable genome can serve as a double-edged sword by providing survival advantages in the ability to evade checkpoint signaling, but also creating vulnerabilities through dependency on alternative genomic maintenance factors. The Fanconi anemia pathway comprises an intricate network of DNA damage signaling and repair that are critical for protection against genomic instability. The importance of this pathway is underlined by the severity of the cancer predisposing syndrome Fanconi anemia which can be caused by biallelic mutations in any one of the 21 genes known thus far. This review delineates the roles of the Fanconi anemia pathway and the molecular actions of Fanconi anemia proteins in confronting replicative, oxidative, and mitotic stress.

Published

2017

22. Damage-dependent regulation of MUS81-EME1 by Fanconi anemia complementation group A protein

Author

Richard S. Myers, Leizhen Wei, Fenghua Yuan, Jennifer J. Hu, Yanbin Zhang, Li Lan, Anaid Benitez, Liangyue Qian, and Satoshi Nakajima

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Fanconi anemia, complementation group C, DNA damage, Genome Integrity, Repair and Replication, Biology, 03 medical and health sciences, Endonuclease, chemistry.chemical_compound, 0302 clinical medicine, Fanconi anemia, hemic and lymphatic diseases, Genetics, medicine, Humans, 030304 developmental biology, 0303 health sciences, Endodeoxyribonucleases, Fanconi Anemia Complementation Group A Protein, nutritional and metabolic diseases, Endonucleases, medicine.disease, Molecular biology, MUS81, FANCA, DNA-Binding Proteins, Cross-Linking Reagents, chemistry, 030220 oncology & carcinogenesis, biology.protein, Methoxsalen, Deoxyribonuclease I, DNA, DNA Damage

Abstract

MUS81-EME1 is a DNA endonuclease involved in replication-coupled repair of DNA interstrand cross-links (ICLs). A prevalent hypothetical role of MUS81-EME1 in ICL repair is to unhook the damage by incising the leading strand at the 3' side of an ICL lesion. In this study, we report that purified MUS81-EME1 incises DNA at the 5' side of a psoralen ICL residing in fork structures. Intriguingly, ICL repair protein, Fanconi anemia complementation group A protein (FANCA), greatly enhances MUS81-EME1-mediated ICL incision. On the contrary, FANCA exhibits a two-phase incision regulation when DNA is undamaged or the damage affects only one DNA strand. Studies using truncated FANCA proteins indicate that both the N- and C-moieties of the protein are required for the incision regulation. Using laser-induced psoralen ICL formation in cells, we find that FANCA interacts with and recruits MUS81 to ICL lesions. This report clarifies the incision specificity of MUS81-EME1 on ICL damage and establishes that FANCA regulates the incision activity of MUS81-EME1 in a damage-dependent manner.

Published

2013

23. Mouse DNA polymerase kappa has a functional role in the repair of DNA strand breaks

Author

Fenghua Yuan, Tie-Shan Tang, Liangyue Qian, Qian Chen, Benjamin P C Chen, Lingna Lv, Yeran Yang, Yanbin Zhang, Yan Jia, Ting Zhang, Xiuli Zhang, Hui Zhang, Yun Wang, Errol C. Friedberg, and Caixia Guo

Subjects

DNA Repair, DNA repair, DNA polymerase, DNA damage, DNA polymerase II, Nuclear Localization Signals, DNA-Directed DNA Polymerase, Biochemistry, Article, Cell Line, Mice, Proliferating Cell Nuclear Antigen, Animals, DNA Breaks, Double-Stranded, DNA Breaks, Single-Stranded, DNA Polymerase Kappa, Molecular Biology, Embryonic Stem Cells, Mice, Knockout, DNA clamp, biology, Lasers, DNA replication, Hydrogen Peroxide, Cell Biology, Molecular biology, Protein Structure, Tertiary, Proliferating cell nuclear antigen, DNA-Binding Proteins, Oxidative Stress, MutS Homolog 2 Protein, biology.protein

Abstract

The Y-family of DNA polymerases support of translesion DNA synthesis (TLS) associated with stalled DNA replication by DNA damage. Recently, a number of studies suggest that some specialized TLS polymerases also support other aspects of DNA metabolism beyond TLS in vivo. Here we show that mouse polymerase kappa (Polκ) could accumulate at laser-induced sites of damage in vivo resembling polymerases eta and iota. The recruitment was mediated through Polκ C-terminus which contains the PCNA-interacting peptide, ubiquitin zinc finger motif 2 and nuclear localization signal. Interestingly, this recruitment was significantly reduced in MSH2-deficient LoVo cells and Rad18-depleted cells. We further observed that Polκ-deficient mouse embryo fibroblasts were abnormally sensitive to H2O2 treatment and displayed defects in both single-strand break repair and double-strand break repair. We speculate that Polκ may have an important role in strand break repair following oxidative stress in vivo.

Published

2013

24. Characterization of ATPase Activity of P2RX2 Cation Channel

Author

Qing Chang, Denise Yan, Prem P. Chapagain, Bechara Kachar, Xue Z. Liu, Yanbin Zhang, Fenghua Yuan, Xi Lin, Amjad Farooq, Rahul Mittal, M'hamed Grati, and Miloslav Sedlacek

Subjects

0301 basic medicine, Physiology, Gating, ATPase activity, lcsh:Physiology, 03 medical and health sciences, ATP hydrolysis, Physiology (medical), medicine, Mechanotransduction, computer modeling, Original Research, Ligand-gated ion channels, lcsh:QP1-981, biology, Purinergic receptor, Cell biology, Calcium ATPase, Electrophysiology, 030104 developmental biology, medicine.anatomical_structure, P2X2, biology.protein, Ligand-gated ion channel, Hair cell, ATP synthase alpha/beta subunits

Abstract

P2X purinergic receptors are plasma membrane ATP-dependent cation channels that are broadly distributed in the mammalian tissues. P2RX2 is a modulator of auditory sensory hair cell mechanotransduction and plays an important role in hair cell tolerance to noise. In this study, we demonstrate for the first time in vitro and in cochlear neuroepithelium, that P2RX2 possesses the ATPase activity. We observed that the P2RX2 V60L human deafness mutation alters its ability to bind ATP, while the G353R has no effect on ATP binding or hydrolysis. A non-hydrolysable ATP assay using HEK293 cells suggests that ATP hydrolysis plays a significant role in the opening and gating of the P2RX2 ion channel. Moreover, the results of structural modeling of the molecule was in agreement with our experimental observations. These novel findings suggest the intrinsic ATPase activity of P2RX2 and provide molecular insights into the channel opening.

Published

2016

25. The Werner Syndrome Protein Promotes CAG/CTG Repeat Stability by Resolving Large (CAG) /(CTG) Hairpins

Author

Amrita Machwe, Tianyi Zhang, Nelson L.S. Chan, Caixia Hou, Guo Min Li, Liya Gu, Jian Huang, David K. Orren, and Fenghua Yuan

Subjects

DNA Replication, musculoskeletal diseases, Exonuclease, congenital, hereditary, and neonatal diseases and abnormalities, Werner Syndrome Helicase, DNA polymerase, DNA repair, macromolecular substances, DNA and Chromosomes, Biochemistry, chemistry.chemical_compound, Humans, education, Molecular Biology, DNA Polymerase III, education.field_of_study, RecQ Helicases, biology, Inverted Repeat Sequences, DNA replication, Helicase, DNA, Cell Biology, Molecular biology, nervous system diseases, carbohydrates (lipids), Exodeoxyribonucleases, chemistry, biology.protein, bacteria, Trinucleotide Repeat Expansion, Trinucleotide repeat expansion, HeLa Cells

Abstract

Expansion of CAG/CTG repeats causes certain neurological and neurodegenerative disorders, and the formation and subsequent persistence of stable DNA hairpins within these repeats are believed to contribute to CAG/CTG repeat instability. Human cells possess a DNA hairpin repair (HPR) pathway, which removes various (CAG)(n) and (CTG)(n) hairpins in a nick-directed and strand-specific manner. Interestingly, this HPR system processes a (CTG)(n) hairpin on the template DNA strand much less efficiently than a (CAG)(n) hairpin on the same strand (Hou, C., Chan, N. L., Gu, L., and Li, G. M. (2009) Incision-dependent and error-free repair of (CAG)(n)/(CTG)(n) hairpins in human cell extracts. Nat. Struct. Mol. Biol. 16, 869-875), suggesting the involvement of an additional component for (CTG)(n) HPR. To identify this activity, a functional in vitro HPR assay was used to screen partially purified HeLa nuclear fractions for their ability to stimulate (CTG)(n) HPR. We demonstrate here that the stimulating activity is the Werner syndrome protein (WRN). Although WRN contains both a 3'→5' helicase activity and a 3'→5' exonuclease activity, the stimulating activity was found to be the helicase activity, as a WRN helicase mutant failed to enhance (CTG)(n) HPR. Consistently, WRN efficiently unwound large (CTG)(n) hairpins and promoted DNA polymerase δ-catalyzed DNA synthesis using a (CTG)(n) hairpin as a template. We, therefore, conclude that WRN stimulates (CTG)(n) HPR on the template DNA strand by resolving the hairpin so that it can be efficiently used as a template for repair or replicative synthesis.

Published

2012

26. Fanconi Anemia Complementation Group A (FANCA) Protein Has Intrinsic Affinity for Nucleic Acids with Preference for Single-stranded Forms

Author

Jessie Y. Liu, Liangyue Qian, Limin Song, Fenghua Yuan, Yanbin Zhang, Chaitanya Jain, Xinliang Zhao, and Gennaro D'Urso

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Fanconi anemia, complementation group C, Mutation, Missense, DNA, Single-Stranded, DNA and Chromosomes, Biology, Peptide Mapping, Biochemistry, chemistry.chemical_compound, Fanconi anemia, hemic and lymphatic diseases, medicine, Humans, Electrophoretic mobility shift assay, Molecular Biology, Fanconi Anemia Complementation Group A Protein, DNA replication, food and beverages, RNA-Binding Proteins, nutritional and metabolic diseases, RNA, Cell Biology, medicine.disease, Molecular biology, Recombinant Proteins, FANCA, Protein Structure, Tertiary, carbohydrates (lipids), DNA-Binding Proteins, Fanconi Anemia, Amino Acid Substitution, chemistry, Nucleic acid, DNA, Protein Binding

Abstract

The Fanconi anemia complementation group A (FANCA) gene is one of 15 disease-causing genes and has been found to be mutated in ∼60% of Fanconi anemia patients. Using purified protein, we report that human FANCA has intrinsic affinity for nucleic acids. FANCA binds to both single-stranded (ssDNA) and double-stranded (dsDNA) DNAs; however, its affinity for ssDNA is significantly higher than for dsDNA in an electrophoretic mobility shift assay. FANCA also binds to RNA with an intriguingly higher affinity than its DNA counterpart. FANCA requires a certain length of nucleic acids for optimal binding. Using DNA and RNA ladders, we determined that the minimum number of nucleotides required for FANCA recognition is ∼30 for both DNA and RNA. By testing the affinity between FANCA and a variety of DNA structures, we found that a 5′-flap or 5′-tail on DNA facilitates its interaction with FANCA. A patient-derived FANCA truncation mutant (Q772X) has diminished affinity for both DNA and RNA. In contrast, the complementing C-terminal fragment of Q772X, C772–1455, retains the differentiated nucleic acid-binding activity (RNA > ssDNA > dsDNA), indicating that the nucleic acid-binding domain of FANCA is located primarily at its C terminus, where most disease-causing mutations are found.

Published

2012

27. FANCA Promotes DNA Double-Strand Break Repair by Catalyzing Single-Strand Annealing and Strand Exchange

Author

Fenghua Yuan, Anna Kim, Kevin Zheng, Alexander V. Mazin, Yu Zhang, Yanbin Zhang, Guanying Wang, Kevin An, Xin Hai Pei, Jaewon Moon, Anna Palovcak, Feng Bai, Wenjun Liu, and Anaid Benitez

Subjects

0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, DNA End-Joining Repair, Genetic Vectors, RAD52, Gene Expression, Moths, Biology, DNA Mismatch Repair, Article, 03 medical and health sciences, FANCG, Fanconi anemia, Cell Line, Tumor, hemic and lymphatic diseases, FANCD2, medicine, Animals, Humans, Monoubiquitination, DNA Breaks, Double-Stranded, Cloning, Molecular, Fanconi Anemia Complementation Group G Protein, Molecular Biology, Osteoblasts, Fanconi Anemia Complementation Group A Protein, Recombinational DNA Repair, nutritional and metabolic diseases, Epithelial Cells, DNA, Cell Biology, medicine.disease, Fanconi Anemia Complementation Group Proteins, Recombinant Proteins, Double Strand Break Repair, FANCA, Rad52 DNA Repair and Recombination Protein, FANCB, Cell biology, 030104 developmental biology, Baculoviridae

Abstract

FANCA is a component of the Fanconi anemia (FA) core complex that activates DNA interstrand crosslink repair by monoubiquitination of FANCD2. Here, we report that purified FANCA protein catalyzes bidirectional single-strand annealing (SA) and strand exchange (SE) at a level comparable to RAD52, while a disease-causing FANCA mutant, F1263Δ, is defective in both activities. FANCG, which directly interacts with FANCA, dramatically stimulates its SA and SE activities. Alternatively, FANCB, which does not directly interact with FANCA, does not stimulate this activity. Importantly, five other patient-derived FANCA mutants also exhibit deficient SA and SE, suggesting that the biochemical activities of FANCA are relevant to the etiology of FA. A cell-based DNA double strand break (DSB) repair assay demonstrates that FANCA plays a direct role in the single-strand annealing sub-pathway (SSA) of DSB repair by catalyzing SA, and this role is independent of the canonical FA pathway and RAD52.

Published

2018

28. FANCI Protein Binds to DNA and Interacts with FANCD2 to Recognize Branched Structures

Author

Wen Zhou, Jimmy El Hokayem, Yanbin Zhang, and Fenghua Yuan

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Fanconi anemia, complementation group C, DNA Repair, DNA repair, Gene Expression, Plasma protein binding, Spodoptera, Biology, Biochemistry, law.invention, chemistry.chemical_compound, law, hemic and lymphatic diseases, Animals, Humans, Point Mutation, Molecular Biology, Fanconi Anemia Complementation Group D2 Protein, Point mutation, DNA, Cell Biology, DNA-binding domain, Molecular biology, Fanconi Anemia Complementation Group Proteins, Recombinant Proteins, Protein Structure, Tertiary, Proliferating cell nuclear antigen, Amino Acid Substitution, chemistry, DNA: Replication, Repair, Recombination, and Chromosome Dynamics, biology.protein, Recombinant DNA, HeLa Cells, Protein Binding

Abstract

In this study, we report that the purified wild-type FANCI (Fanconi anemia complementation group I) protein directly binds to a variety of DNA substrates. The DNA binding domain roughly encompasses residues 200-1000, as suggested by the truncation study. When co-expressed in insect cells, a small fraction of FANCI forms a stable complex with FANCD2 (Fanconi anemia complementation group D2). Intriguingly, the purified FANCI-FANCD2 complex preferentially binds to the branched DNA structures when compared with either FANCI or FANCD2 alone. Co-immunoprecipitation with purified proteins indicates that FANCI interacts with FANCD2 through its C-terminal amino acid 1001-1328 fragment. Although the C terminus of FANCI is dispensable for direct DNA binding, it seems to be involved in the regulation of DNA binding activity. This notion is further enhanced by two C-terminal point mutations, R1285Q and D1301A, which showed differentiated DNA binding activity. We also demonstrate that FANCI forms discrete nuclear foci in HeLa cells in the absence or presence of exogenous DNA damage. The FANCI foci are colocalized perfectly with FANCD2 and partially with proliferating cell nuclear antigen irrespective of mitomycin C treatment. An increased number of FANCI foci form and become resistant to Triton X extraction in response to mitomycin C treatment. Our data suggest that the FANCI-FANCD2 complex may participate in repair of damaged replication forks through its preferential recognition of branched structures.

Published

2009

29. Identification and characterization of OGG1 mutations in patients with Alzheimer's disease

Author

Bei Bei Zhu, Mark A. Lovell, Jian Huang, Liya Gu, Fenghua Yuan, Maxwell P. Lee, William R. Markesbery, Yanbin Zhang, Xiaoyu Pan, Guo Min Li, and Guogen Mao

Subjects

Molecular Sequence Data, Biology, medicine.disease_cause, DNA Glycosylases, Pathogenesis, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Alzheimer Disease, Genetics, medicine, Humans, Point Mutation, Amino Acid Sequence, Gene, Peptide sequence, Molecular Biology, 030304 developmental biology, 0303 health sciences, Mutation, Base Sequence, Point mutation, Brain, medicine.disease, Molecular biology, 3. Good health, chemistry, Amino Acid Substitution, DNA glycosylase, Alzheimer's disease, 030217 neurology & neurosurgery, DNA

Abstract

Patients with Alzheimer's disease (AD) exhibit higher levels of 8-oxo-guanine (8-oxoG) DNA lesions in their brain, suggesting a reduced or defective 8-oxoG repair. To test this hypothesis, this study investigated 14 AD patients and 10 age-matched controls for mutations of the major 8-oxoG removal gene OGG1. Whereas no alterations were detected in any control samples, four AD patients exhibited mutations in OGG1, two carried a common single base (C796) deletion that alters the carboxyl terminal sequence of OGG1, and the other two had nucleotide alterations leading to single amino acid substitutions. In vitro biochemical assays revealed that the protein encoded by the C796-deleted OGG1 completely lost its 8-oxoG glycosylase activity, and that the two single residue-substituted OGG1 proteins showed a significant reduction in the glycosylase activity. These results were consistent with the fact that nuclear extracts derived from a limited number of AD patients with OGG1 mutations exhibited greatly reduced 8-oxoG glycosylase activity compared with age-matched controls and AD patients without OGG1 alterations. Our findings suggest that defects in OGG1 may be important in the pathogenesis of AD in a significant fraction of AD patients and provide new insight into the molecular basis for the disease.

Published

2007

30. Reconstitution of 5′-Directed Human Mismatch Repair in a Purified System

Author

Fenghua Yuan, Alan E. Tomkinson, Steven R. Presnell, Keli Tian, Yin Gao, Guo Min Li, Liya Gu, and Yanbin Zhang

Subjects

DNA Ligases, DNA Repair, 5' Flanking Region, Base Pair Mismatch, Biology, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Exonuclease 1, DNA Ligase ATP, 0302 clinical medicine, Replication Protein A, Humans, HMGB1 Protein, Human proteins, Polymerase, 030304 developmental biology, Genetics, chemistry.chemical_classification, 0303 health sciences, DNA ligase, Cell-Free System, Biochemistry, Genetics and Molecular Biology(all), Processivity, Proliferating cell nuclear antigen, Cell biology, Neoplasm Proteins, DNA-Binding Proteins, DNA Repair Enzymes, Exodeoxyribonucleases, MutL Proteins, chemistry, 030220 oncology & carcinogenesis, biology.protein, DNA mismatch repair, Nucleotide excision repair

Abstract

This paper reports reconstitution of 5'-nick-directed mismatch repair using purified human proteins. The reconstituted system includes MutSalpha or MutSbeta, MutLalpha, RPA, EXO1, HMGB1, PCNA, RFC, polymerase delta, and ligase I. In this system, MutSbeta plays a limited role in repair of base-base mismatches, but it processes insertion/deletion mispairs much more efficiently than MutSalpha, which efficiently corrects both types of heteroduplexes. MutLalpha reduces the processivity of EXO1 and terminates EXO1-catalyzed excision upon mismatch removal. In the absence of MutLalpha, mismatch-provoked excision by EXO1 occurs extensively. RPA and HMGB1 play similar but complementary roles in stimulating MutSalpha-activated, EXO1-catalyzed excision in the presence of a mismatch, but RPA has a distinct role in facilitating MutLalpha-mediated excision termination past mismatch. Evidence is provided that efficient repair of a single mismatch requires multiple molecules of MutSalpha-MutLalpha complex. These data suggest a model for human mismatch repair involving coordinated initiation and termination of mismatch-provoked excision.

Published

2005

31. Stimulation of Hepatitis C Virus (HCV) Nonstructural Protein 3 (NS3) Helicase Activity by the NS3 Protease Domain and by HCV RNA-Dependent RNA Polymerase

Author

C. Cheng Kao, Ranjith Kumar, Guangxiang Luo, Chen Zhang, Fenghua Yuan, Zhaohui Cai, Young Chan Kim, and Pei Yong Shi

Subjects

viruses, Hepatitis C virus, medicine.medical_treatment, Immunology, Viral Nonstructural Proteins, Biology, medicine.disease_cause, Microbiology, chemistry.chemical_compound, Virology, RNA polymerase, medicine, NS5B, NS3, Protease, Serine Endopeptidases, virus diseases, Helicase, biochemical phenomena, metabolism, and nutrition, RNA Helicase A, Molecular biology, Recombinant Proteins, digestive system diseases, Genome Replication and Regulation of Viral Gene Expression, NS2-3 protease, Spectrometry, Fluorescence, chemistry, Insect Science, biology.protein, RNA, Viral, RNA Helicases

Abstract

Hepatitis C virus (HCV) nonstructural protein 3 (NS3) possesses multiple enzyme activities. The N-terminal one-third of NS3 primarily functions as a serine protease, while the remaining two-thirds of NS3 serve as a helicase and nucleoside triphosphatase. Whether the multiple enzyme activities of NS3 are functionally interdependent and/or modulated by other viral NS proteins remains unclear. We performed biochemical studies to examine the functional interdependence of the NS3 protease and helicase domains and the modulation of NS3 helicase by NS5B, an RNA-dependent RNA polymerase (RdRp). We found that the NS3 protease domain of the full-length NS3 (NS3FL) enhances the NS3 helicase activity. Additionally, HCV RdRp stimulates the NS3FL helicase activity by more than sevenfold. However, the helicase activity of the NS3 helicase domain was unaffected by HCV RdRp. Glutathione S -transferase pull-down as well as fluorescence anisotropy results revealed that the NS3 protease domain is required for specific NS3 and NS5B interaction. These findings suggest that HCV RdRp regulates the functions of NS3 during HCV replication. In contrast, NS3FL does not increase NS5B RdRp activity in vitro, which is contrary to a previously published report that the HCV NS3 enhances NS5B RdRp activity.

Published

2005

32. Evidence for Involvement of HMGB1 Protein in Human DNA Mismatch Repair

Author

Fenghua Yuan, Liya Gu, Shuangli Guo, Guo Min Li, and Chunmei Wang

Subjects

Base Pair Mismatch, DNA damage, Molecular Sequence Data, Biology, HMGB1, Biochemistry, Substrate Specificity, HeLa, MutS-1, Humans, Nucleotide, Amino Acid Sequence, HMGB1 Protein, Molecular Biology, Cell Nucleus, chemistry.chemical_classification, Cell Biology, biology.organism_classification, Molecular biology, Peptide Fragments, Cell biology, DNA-Binding Proteins, High-mobility group, chemistry, HMG-Box Domains, MutS Homolog 3 Protein, biology.protein, DNA mismatch repair, HeLa Cells, Nucleotide excision repair

Abstract

Defects in human DNA mismatch repair predispose to cancer, but many components of the pathway have not been identified. We report here the identification and characterization of a novel component required for mismatch repair in human cells. A 30-kDa protein was purified to homogeneity by virtue of its ability to complement a depleted HeLa extract in repair of mismatched heteroduplexes. The complementing activity was identified as HMGB1 (the high mobility group box 1 protein), a non-histone chromatin protein that facilitates protein-protein interactions and recognizes DNA damage. Evidence is also presented that HMGB1 physically interacts with MutSalpha and is required at a step prior to the excision of mispaired nucleotide in mismatch repair.

Published

2004

33. Differential Requirement for Proliferating Cell Nuclear Antigen in 5′ and 3′ Nick-directed Excision in Human Mismatch Repair

Author

Steven R. Presnell, Shuangli Guo, Liya Gu, Fenghua Yuan, Yanbin Zhang, and Guo Min Li

Subjects

Cyclin-Dependent Kinase Inhibitor p21, DNA, Complementary, DNA Repair, Base Pair Mismatch, MutS DNA Mismatch-Binding Protein, DNA repair, Recombinant Fusion Proteins, Molecular Sequence Data, Biology, Biochemistry, Bacterial Proteins, Cyclins, Proliferating Cell Nuclear Antigen, Escherichia coli, medicine, Humans, Molecular Biology, Glutathione Transferase, Adenosine Triphosphatases, Cell Nucleus, Base Sequence, Dose-Response Relationship, Drug, Escherichia coli Proteins, DNA, Cell Biology, Molecular biology, Fusion protein, Protein Structure, Tertiary, Proliferating cell nuclear antigen, DNA-Binding Proteins, Blot, Blotting, Southern, Cell nucleus, medicine.anatomical_structure, biology.protein, DNA mismatch repair, HeLa Cells

Abstract

Proliferating cell nuclear antigen (PCNA) is involved in mammalian mismatch repair at a step prior to or at mismatch excision, but the molecular mechanism of this process is not fully understood. To examine the role of PCNA in mismatch-provoked and nick-directed excision, orientation-specific mismatch removal of heteroduplexes with a pre-existing nick was monitored in human nuclear extracts supplemented with the PCNA inhibitor protein p21. We show here that, whereas 3' nick-directed mismatch excision was completely inhibited by low concentrations of p21 or a p21 C-terminal fusion protein, 5' nick-directed excision was only partially blocked under the same conditions. No further reduction of the 5' excision was detected when a much higher concentration of p21 C-terminal protein was used. These results suggest the following. (i) There is a differential requirement for PCNA in 3' and 5' nick-directed excision; and (ii) 5' nick-directed excision is conducted by a manner either dependent on or independent of PCNA. Our in vitro reconstitution experiments indeed identified a 5' nick-directed excision pathway that is dependent on PCNA, hMutSalpha, and a partially purified fraction from a HeLa nuclear extract.

Published

2004

34. Crystal structure of a Fanconi anemia-associated nuclease homolog bound to 5′ flap DNA: basis of interstrand cross-link repair by FAN1

Author

Anthony M. Carr, Aera Jo, Fenghua Yuan, Gwang Hyeon Gwon, Yanbin Zhang, Yunje Cho, Youngchang Kim, Adam T. Watson, Youngran Kim, Yaqi Liu, and Thomas J. Etheridge

Subjects

Models, Molecular, Flap Endonucleases, Biology, Q1, chemistry.chemical_compound, Fanconi anemia, hemic and lymphatic diseases, Catalytic Domain, Genetics, medicine, Holliday junction, Humans, Flap endonuclease, Gene, QD0415, Nuclease, FAN1, medicine.disease, Molecular biology, Protein Structure, Tertiary, Exodeoxyribonucleases, chemistry, Pseudomonas aeruginosa, biology.protein, Interstrand cross-link repair, Crystallization, DNA, Research Paper, Protein Binding, Developmental Biology

Abstract

Fanconi anemia (FA) is an autosomal recessive genetic disorder caused by defects in any of 15 FA genes responsible for processing DNA interstrand cross-links (ICLs). The ultimate outcome of the FA pathway is resolution of cross-links, which requires structure-selective nucleases. FA-associated nuclease 1 (FAN1) is believed to be recruited to lesions by a monoubiquitinated FANCI–FANCD2 (ID) complex and participates in ICL repair. Here, we determined the crystal structure of Pseudomonas aeruginosa FAN1 (PaFAN1) lacking the UBZ (ubiquitin-binding zinc) domain in complex with 5′ flap DNA. All four domains of the right-hand-shaped PaFAN1 are involved in DNA recognition, with each domain playing a specific role in bending DNA at the nick. The six-helix bundle that binds the junction connects to the catalytic viral replication and repair (VRR) nuclease (VRR nuc) domain, enabling FAN1 to incise the scissile phosphate a few bases distant from the junction. The six-helix bundle also inhibits the cleavage of intact Holliday junctions. PaFAN1 shares several conserved features with other flap structure-selective nucleases despite structural differences. A clamping motion of the domains around the wedge helix, which acts as a pivot, facilitates nucleolytic cleavage. The PaFAN1 structure provides insights into how archaeal Holliday junction resolvases evolved to incise 5′ flap substrates and how FAN1 integrates with the FA complex to participate in ICL repair.

Published

2014

35. Full-range Fourier domain Doppler optical coherence tomography based on sinusoidal phase modulation

Author

Fenghua Yuan, Peng Bu, Zhongliang Li, Nan Nan, Chen Yan, Osami Sasaki, Wang Xuan, Xin Guo, and Xiangzhao Wang

Subjects

Phase (waves), Sensitivity and Specificity, symbols.namesake, Mice, Optics, Optical coherence tomography, Image Interpretation, Computer-Assisted, medicine, Laser-Doppler Flowmetry, Animals, Electrical and Electronic Engineering, Engineering (miscellaneous), Optical path length, Physics, medicine.diagnostic_test, business.industry, Reproducibility of Results, Ear, Equipment Design, Atomic and Molecular Physics, and Optics, Equipment Failure Analysis, Fourier transform, Flow velocity, symbols, Spatial frequency, business, Phase modulation, Doppler effect, Blood Flow Velocity, Tomography, Optical Coherence

Abstract

A novel full-range Fourier domain Doppler optical coherence tomography (full-range FD-DOCT) using sinusoidal phase modulation for B-M scan is proposed. In this sinusoidal B-M scan, zero optical path difference (OPD) position does not move corresponding to lateral scanning points in contrast to linear B-M scan. Since high phase sensitivity arises around the zero OPD position, the proposed full-range FD-DOCT can achieve easily high velocity sensitivity without mirror image around the zero OPD position. Velocity sensitivity dependent on the OPD and the interval of scanning points is examined, and flow velocity detection capability is verified through Doppler imaging of a flow phantom and an in vivo biological sample.

Published

2014

36. Error-free and error-prone lesion bypass by human DNA polymerase kappa in vitro

Author

Xiaohua Wu, Zhigang Wang, Nicholas E. Geacintov, Fenghua Yuan, Mu Wang, Olga Rechkoblit, Yanbin Zhang, and John-Stephen Taylor

Subjects

Guanine, Base Pair Mismatch, DNA damage, DNA polymerase, Recombinant Fusion Proteins, Pyrimidine dimer, DNA-Directed DNA Polymerase, Article, Catalysis, Substrate Specificity, Lesion, DNA Adducts, chemistry.chemical_compound, Benzo(a)pyrene, Genetics, medicine, Humans, AP site, DNA Polymerase Kappa, Polymerase, Base Sequence, biology, Nucleotides, Proteins, Templates, Genetic, 2-Acetylaminofluorene, Molecular biology, chemistry, Mutagenesis, Pyrimidine Dimers, biology.protein, medicine.symptom, DNA, DNA Damage, Mutagens

Abstract

Error-free lesion bypass and error-prone lesion bypass are important cellular responses to DNA damage during replication, both of which require a DNA polymerase (Pol). To identify lesion bypass DNA polymerases, we have purified human Polkappa encoded by the DINB1 gene and examined its response to damaged DNA templates. Here, we show that human Polkappa is a novel lesion bypass polymerase in vitro. Purified human Polkappa efficiently bypassed a template 8-oxoguanine, incorporating mainly A and less frequently C opposite the lesion. Human Polkappa most frequently incorporated A opposite a template abasic site. Efficient further extension required T as the next template base, and was mediated mainly by a one-nucleotide deletion mechanism. Human Polkappa was able to bypass an acetylaminofluorene-modified G in DNA, incorporating either C or T, and less efficiently A opposite the lesion. Furthermore, human Polkappa effectively bypassed a template (-)-trans-anti-benzo[a]pyrene-N:(2)-dG lesion in an error-free manner by incorporating a C opposite the bulky adduct. In contrast, human Polkappa was unable to bypass a template TT dimer or a TT (6-4) photoproduct, two of the major UV lesions. These results suggest that Polkappa plays an important role in both error-free and error-prone lesion bypass in humans.

Published

2000

37. Human DNA polymerase kappa synthesizes DNA with extraordinarily low fidelity

Author

Fenghua Yuan, Zhigang Wang, Deepak K. Rajpal, Hua Xin, Danzhou Yang, Xiaohua Wu, and Yanbin Zhang

Subjects

Base Pair Mismatch, DNA damage, DNA polymerase, Base pair, DNA polymerase beta, DNA-Directed DNA Polymerase, Article, Substrate Specificity, chemistry.chemical_compound, Genetics, Humans, Base Pairing, DNA Polymerase beta, Polymerase, Base Sequence, DNA synthesis, biology, Nucleotides, Mutagenesis, Proteins, DNA, Templates, Genetic, Kinetics, chemistry, DNA Polymerase iota, biology.protein, Thermodynamics, DNA Damage

Abstract

Escherichia coli DNA polymerase IV encoded by the dinB gene is involved in untargeted mutagenesis. Its human homologue is DNA polymerase kappa (Polkappa) encoded by the DINB1 gene. Our recent studies have indicated that human Polkappa is capable of both error-free and error-prone translesion DNA synthesis in vitro. However, it is not known whether human Polkappa also plays a role in untargeted mutagenesis. To examine this possibility, we have measured the fidelity of human Polkappa during DNA synthesis from undamaged templates. Using kinetic measurements of nucleotide incorporations and a fidelity assay with gapped M13mp2 DNA, we show that human Polkappa synthesizes DNA with extraordinarily low fidelity. At the lacZalpha target gene, human Polkappa made on average one error for every 200 nucleotides synthesized, with a predominant T--G transversion mutation at a rate of 1/147. The overall error rate of human Polkappa is 1.7-fold lower than human Poleta, but 33-fold higher than human Polbeta, a DNA polymerase with very low fidelity. Thus, human Polkappa is one of the most inaccurate DNA polymerases known. These results support a role for human Polkappa in untargeted mutagenesis surrounding a DNA lesion and in DNA regions without damage.

Published

2000

38. Preferential Incorporation of G Opposite Template T by the Low-Fidelity Human DNA Polymerase ι

Author

Fenghua Yuan, Xiaohua Wu, Zhigang Wang, and Yanbin Zhang

Subjects

DNA Replication, DNA polymerase, Base pair, Stereochemistry, DNA-Directed DNA Polymerase, Substrate Specificity, chemistry.chemical_compound, Humans, Thymine Nucleotides, AP site, Base Pairing, Molecular Biology, Polymerase, DNA clamp, biology, DNA replication, Templates, Genetic, Cell Biology, DNA Dynamics and Chromosome Structure, Molecular biology, Kinetics, chemistry, Genetic Code, Mutagenesis, DNA Polymerase iota, biology.protein, Guanosine Triphosphate, DNA Polymerase Iota, DNA

Abstract

DNA polymerase activity is essential for replication, recombination, repair, and mutagenesis. All DNA polymerases studied so far from any biological source synthesize DNA by the Watson-Crick base-pairing rule, incorporating A, G, C, and T opposite the templates T, C, G, and A, respectively. Non-Watson-Crick base pairs would lead to mutations. In this report, we describe the ninth human DNA polymerase, Pol(iota), encoded by the RAD30B gene. We show that human Pol(iota) violates the Watson-Crick base-pairing rule opposite template T. During base selection, human Pol(iota) preferred T-G base pairing, leading to G incorporation opposite template T. The resulting T-G base pair was less efficiently extended by human Pol(iota) compared to the Watson-Crick base pairs. Consequently, DNA synthesis frequently aborted opposite template T, a property we designated the T stop. This T stop restricted human Pol(iota) to a very short stretch of DNA synthesis. Furthermore, kinetic analyses show that human Pol(iota) copies template C with extraordinarily low fidelity, misincorporating T, A, and C with unprecedented frequencies of 1/9, 1/10, and 1/11, respectively. Human Pol(iota) incorporated one nucleotide opposite a template abasic site more efficiently than opposite a template T, suggesting a role for human Pol(iota) in DNA lesion bypass. The unique features of preferential G incorporation opposite template T and T stop suggest that DNA Pol(iota) may additionally play a specialized function in human biology.

Published

2000

39. The human REV1 gene codes for a DNA template-dependent dCMP transferase

Author

Fenghua Yuan, Wensheng Lin, Xiaohua Wu, Yanbin Zhang, Hua Xin, and Zhigang Wang

Subjects

DNA, Complementary, Saccharomyces cerevisiae Proteins, DNA damage, Cloning, Organism, Molecular Sequence Data, Saccharomyces cerevisiae, Biology, medicine.disease_cause, Fungal Proteins, chemistry.chemical_compound, Complementary DNA, Genetics, medicine, Humans, AP site, Amino Acid Sequence, Gene, Conserved Sequence, Mutation, Sequence Homology, Amino Acid, Mutagenesis, Chromosome Mapping, Deoxycytidine Monophosphate, Templates, Genetic, Nucleotidyltransferases, chemistry, Biochemistry, Chromosomes, Human, Pair 2, REV1, DNA, Research Article

Abstract

DNA is frequently damaged by various physical and chemical agents. DNA damage can lead to mutations during replication. In the yeast Saccharomyces cerevisiae, the damage-induced mutagenesis pathway requires the Rev1 protein. We have isolated a human cDNA homologous to the yeast REV1 gene. The human REV1 cDNA consists of 4255 bp and codes for a protein of 1251 amino acid residues with a calculated molecular weight of 138 248 Da. The human REV1 gene is localized between 2q11.1 and 2q11.2. We show that the human REV1 protein is a dCMP transferase that specifically inserts a dCMP residue opposite a DNA template G. In addition, the human REV1 transferase is able to efficiently and specifically insert a dCMP opposite a DNA template apurinic/apyrimidinic (AP) site or a uracil residue. These results suggest that the REV1 transferase may play a critical role during mutagenic translesion DNA synthesis bypassing a template AP site in human cells. Consistent with its role as a fundamental mutagenic protein, the REV1 gene is ubiquitously expressed in various human tissues.

Published

1999

40. Coordinated Processing of 3′ Slipped (CAG)n/(CTG)n Hairpins by DNA Polymerases β and δ Preferentially Induces Repeat Expansions*

Author

Guogen Mao, Caixia Hou, Jinzhen Guo, Yanbin Zhang, Liya Gu, Jian Huang, Fenghua Yuan, Tianyi Zhang, Guo Min Li, Nelson L.S. Chan, and Jianxin Wu

Subjects

musculoskeletal diseases, DNA Replication, congenital, hereditary, and neonatal diseases and abnormalities, DNA polymerase, Inverted Repeat Sequences, DNA polymerase II, DNA and Chromosomes, Biochemistry, DNA polymerase delta, mental disorders, Humans, Molecular Biology, DNA Polymerase beta, DNA Polymerase III, biology, DNA replication, Cell Biology, Processivity, DNA, Molecular biology, nervous system diseases, biology.protein, Primer (molecular biology), Trinucleotide repeat expansion, HeLa Cells

Abstract

Expansion of CAG/CTG trinucleotide repeats causes certain familial neurological disorders. Hairpin formation in the nascent strand during DNA synthesis is considered a major path for CAG/CTG repeat expansion. However, the underlying mechanism is unclear. We show here that removal or retention of a nascent strand hairpin during DNA synthesis depends on hairpin structures and types of DNA polymerases. Polymerase (pol) δ alone removes the 3′-slipped hairpin using its 3′-5′ proofreading activity when the hairpin contains no immediate 3′ complementary sequences. However, in the presence of pol β, pol δ preferentially facilitates hairpin retention regardless of hairpin structures. In this reaction, pol β incorporates several nucleotides to the hairpin 3′-end, which serves as an effective primer for the continuous DNA synthesis by pol δ, thereby leading to hairpin retention and repeat expansion. These findings strongly suggest that coordinated processing of 3′-slipped (CAG)n/(CTG)n hairpins by polymerases δ and β on during DNA synthesis induces CAG/CTG repeat expansions. Background: Expansion of CAG/CTG repeats causes familial neurological disorders, but the molecular basis is unknown. Results: DNA polymerases β and δ effectively incorporate nucleotides to a CAG/CTG hairpin primer, leading to hairpin retention. Conclusion: Coordinated actions by polymerases β and δ on hairpin primers during DNA synthesis promotes CAG/CTG repeat expansions. Significance: The work discovers a novel mechanism for CAG/CTG repeat expansions.

Published

2013

41. Eukaryotic DNA mismatch repair in vitro

Author

Fenghua, Yuan, Limin, Song, Fengsong, Liu, Liya, Gu, and Yanbin, Zhang

Subjects

Cell Nucleus, Base Sequence, Cytological Techniques, Humans, Saccharomyces cerevisiae, DNA, Fungal, DNA Mismatch Repair, HeLa Cells

Abstract

Mismatch repair corrects biosynthetic errors generated during DNA replication. Mismatch repair deficiency causes a mutator phenotype and directly underlies hereditary nonpolyposis colorectal cancer and some sporadic cancers. Because of remarkably high conservation of the mismatch repair machinery between the budding yeast (Saccharomyces cerevisiae) and humans, the study of mismatch repair in yeast has provided tremendous insights into the mechanisms of this repair pathway in humans. Here we describe a set of practical protocols for how to prepare the yeast and HeLa cell-free nuclear extracts and site-specific DNA mismatch substrates, and how to carry out the in vitro mismatch repair assay. We validated the yeast cell-free system by the mismatch repair deficient strain (Δmsh2) and the complementation assay with purified yeast MutSα.

Published

2012

42. Termination of exonuclease 1‐catalyzed mismatch excision requires physical interaction between exonuclease 1 and MutLα

Author

Liya Gu, Sanghee Lee, Lei Tian, Yanbin Zhang, Fenghua Yuan, Zhanmin Fan, and Guo-Min Li

Subjects

Exonuclease 1, Chemistry, Genetics, Biophysics, Physical interaction, Molecular Biology, Biochemistry, Biotechnology

Published

2012

43. FANCA has intrinsic affinity to nucleic acids with preference for single‐stranded forms

Author

Fenghua Yuan, Xinliang Zhao, Limin Song, Jesse Y. Liu, Liangyue Qian, Chaitanya Jain, Yanbin Zhang, and Gennaro D'Urso

Subjects

Biochemistry, Chemistry, Genetics, Nucleic acid, Molecular Biology, FANCA, Preference, Biotechnology

Published

2012

44. Eukaryotic DNA Mismatch Repair In Vitro

Author

Liya Gu, Yanbin Zhang, Fenghua Yuan, Fengsong Liu, and Limin Song

Subjects

Genetics, Protein-fragment complementation assay, DNA repair, Saccharomyces cerevisiae, DNA replication, biology.protein, Eukaryotic DNA replication, DNA mismatch repair, Biology, biology.organism_classification, Nucleotide excision repair, Cell biology, Proliferating cell nuclear antigen

Abstract

Mismatch repair corrects biosynthetic errors generated during DNA replication. Mismatch repair deficiency causes a mutator phenotype and directly underlies hereditary nonpolyposis colorectal cancer and some sporadic cancers. Because of remarkably high conservation of the mismatch repair machinery between the budding yeast (Saccharomyces cerevisiae) and humans, the study of mismatch repair in yeast has provided tremendous insights into the mechanisms of this repair pathway in humans. Here we describe a set of practical protocols for how to prepare the yeast and HeLa cell-free nuclear extracts and site-specific DNA mismatch substrates, and how to carry out the in vitro mismatch repair assay. We validated the yeast cell-free system by the mismatch repair deficient strain (Δmsh2) and the complementation assay with purified yeast MutSα.

Published

2012

45. Does a helicase activity help mismatch repair in eukaryotes?

Author

Limin Song, Yanbin Zhang, and Fenghua Yuan

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Base Pair Mismatch, Clinical Biochemistry, Eukaryotic DNA replication, complex mixtures, Biochemistry, DNA Mismatch Repair, chemistry.chemical_compound, Genetics, Escherichia coli, Animals, Humans, Molecular Biology, biology, RecQ Helicases, Escherichia coli Proteins, DNA replication, DNA Helicases, Helicase, Eukaryota, Cell Biology, biology.organism_classification, digestive system diseases, Fanconi Anemia Complementation Group Proteins, Basic-Leucine Zipper Transcription Factors, chemistry, biology.protein, DNA mismatch repair, Eukaryote, DNA, Nucleotide excision repair

Abstract

Mismatch repair (MMR) corrects innate DNA replication infidelities. Many components of eukaryotic MMR have been identified, the molecular mechanism of MMR has been largely demonstrated, and furthermore the nick-directed MMR reactions have been reconstituted with purified human proteins in vitro. However, some fundamental questions still remain to be answered. One such question is whether a DNA helicase activity is required for MMR in eukaryotes. This short review presents an overview of the interactions between eukaryotic DNA helicases and MMR factors, and suggests a possible mechanism for how DNA helicases may be involved in repair of DNA mismatches.

Published

2010

46. Measuring strand discontinuity-directed mismatch repair in yeast Saccharomyces cerevisiae by cell-free nuclear extracts

Author

Fangfang Lai, Wen Zhou, Liya Gu, Yanbin Zhang, Jimmy El Hokayem, and Fenghua Yuan

Subjects

Saccharomyces cerevisiae Proteins, DNA Repair, DNA repair, Saccharomyces cerevisiae, DNA Mismatch Repair, General Biochemistry, Genetics and Molecular Biology, Substrate Specificity, Protein-fragment complementation assay, Gene Expression Regulation, Fungal, DNA, Fungal, Molecular Biology, Genetics, Cell Nucleus, biology, Cell-Free System, Genetic Complementation Test, Fungal genetics, DNA replication, Helicase, Reproducibility of Results, biology.organism_classification, Cell biology, DNA-Binding Proteins, Exodeoxyribonucleases, MutS Homolog 2 Protein, biology.protein, DNA mismatch repair, Nucleotide excision repair

Abstract

Mismatch repair corrects biosynthetic errors generated during DNA replication, whose deficiency causes a mutator phenotype and directly underlies hereditary non-polyposis colorectal cancer and sporadic cancers. Because of remarkably high conservation of the mismatch repair machinery between the budding yeast (Saccharomyces cerevisiae) and humans, the study of mismatch repair in yeast has provided tremendous insights into the mechanisms of this repair pathway in humans. In addition, yeast cells possess an unbeatable advantage over human cells in terms of the easy genetic manipulation, the availability of whole genome deletion strains, and the relatively low cost for setting up the system. Although many components of eukaryotic mismatch repair have been identified, it remains unclear if additional factors, such as DNA helicase(s) and redundant nuclease(s) besides EXO1, participate in eukaryotic mismatch repair. To facilitate the discovery of novel mismatch repair factors, we developed a straightforward in vitro cell-free repair system. Here, we describe the practical protocols for preparation of yeast cell-free nuclear extracts and DNA mismatch substrates, and the in vitro mismatch repair assay. The validity of the cell-free system was confirmed by the mismatch repair deficient yeast strain (Deltamsh2) and the complementation assay with purified yeast MSH2-MSH6.

Published

2009

47. The interplay between hMLH1 and hMRE11: role in MMR and the effect of hMLH1 mutations

Author

Liya Gu, Chengtao Her, Shinichi Fukushige, Fengxue Zhu, Nianxi Zhao, Fenghua Yuan, and Anoria K. Haick

Subjects

G2 Phase, congenital, hereditary, and neonatal diseases and abnormalities, DNA Repair, DNA repair, Base Pair Mismatch, Mutant, Biophysics, Mutation, Missense, Biology, Biochemistry, DNA-binding protein, Article, Cell Line, Two-Hybrid System Techniques, medicine, Missense mutation, Humans, Nuclear protein, Molecular Biology, neoplasms, Adaptor Proteins, Signal Transducing, Cisplatin, Genetics, MRE11 Homologue Protein, Nuclear Proteins, Cell Biology, In vitro, digestive system diseases, Peptide Fragments, DNA-Binding Proteins, Cell culture, MutL Protein Homolog 1, Cell Division, medicine.drug

Abstract

Our previous studies indicate that hMRE11 plays a role in MMR, and this function of hMRE11 is most likely mediated by the hMLH1–hMRE11 interaction. Here, we explored the functional implications of the hMLH1–hMRE11 interaction in MMR and the effects of hMLH1 mutations on their interaction. Our in vitro MMR assay demonstrated that the dominant-negative hMRE11452–634 mutant peptide (i.e., harboring only the hMLH1-interacting domain) imparted a significant reduction in both 3′ excision and 3′-directed MMR activities. Furthermore, the expression of hMRE11452–634, and to a lesser extent hMRE111–634 (ATLD1), impaired G2/M checkpoint control in response to MNU and cisplatin treatments, rendering cells resistant to killings by these two anticancer drugs. Analysis of 38 hMLH1 missense mutations showed that the majority of mutations caused significant (>50%) reductions in their interaction with hMRE11, suggesting a potential link between aberrant protein interaction and the pathogenic effects of hMLH1 variants.

Published

2008

48. Identification of regulatory factor X as a novel mismatch repair stimulatory factor

Author

Fenghua Yuan, Liya Gu, Yanbin Zhang, Guo Min Li, and Daojing Wang

Subjects

Regulatory Factor X Transcription Factors, Biochemistry, DNA-binding protein, DNA Mismatch Repair, Catalysis, Mass Spectrometry, law.invention, law, Transcription (biology), medicine, Humans, RNA, Small Interfering, Molecular Biology, Transcription factor, biology, Bare lymphocyte syndrome, Cell Biology, Exons, medicine.disease, Molecular biology, DNA-Binding Proteins, Histone, Acetylation, Multiprotein Complexes, DNA: Replication, Repair, Recombination, and Chromosome Dynamics, biology.protein, Recombinant DNA, DNA mismatch repair, Gene Deletion, HeLa Cells, Transcription Factors

Abstract

This report describes the identification and purification of a novel mismatch repair stimulatory factor from HeLa cell extracts. This activity copurifies with a proliferating cell nuclear antigen-dependent 5 ′ → 3 ′ DNA excision activity during several purification steps but is resolved from the excision activity during gel filtration chromatography using Sephacryl S-300. After purification to near homogeneity, the stimulatory factor is associated with three polypeptides with apparent molecular masses of 68, 36, and 30 kDa. Peptide sequencing analysis by tandem mass spectrometry identified the stimulatory factor as the heterotrimeric regulatory factor X (RFX) complex, which regulates transcription of the class II major histocompatibility complex by facilitating histone acetylation and is defective in the human hereditary immunodeficiency syndrome called bare lymphocyte syndrome. This conclusion was confirmed by the facts that purified recombinant RFX stimulates mismatch repair in an in vitro reconstituted mismatch repair system and that depletion of RFX from nuclear extracts or RFX knockdown in cells reduces mismatch repair activity. As expected, RFX knockdown cells display instability in microsatellite sequences. The possible role of RFX in human MMR repair is discussed.

Published

2008

49. A Lightweight Sensor Network Management System Design

Author

Lei Wang, B. Shirazit, Fenghua Yuan, Nina Peterson, Richard G. LaHusen, Wen-Zhan Song, and Yang Peng

Subjects

Memory management, Intelligent sensor, Emergency management, business.industry, Computer science, Embedded system, Sensor node, Management system, Overhead (computing), Management functions, ComputerSystemsOrganization_SPECIAL-PURPOSEANDAPPLICATION-BASEDSYSTEMS, business, Wireless sensor network

Abstract

In this paper, we propose a lightweight and transparent management framework for TinyOS sensor networks, called L-SNMS, which minimizes the overhead of management functions, including memory usage overhead, network traffic overhead, and integration overhead. We accomplish this by making L-SNMS virtually transparent to other applications hence requiring minimal integration. The proposed L-SNMS framework has been successfully tested on various sensor node platforms, including TelosB, MICAz and IMote2.

Published

2008

50. Preferential loss of mismatch repair function in refractory and relapsed acute myeloid leukemia: potential contribution to AML progression

Author

Fenghua Yuan, Kimberly J. Absher, Liya Gu, Guogen Mao, Craig T. Jordan, Dianna S. Howard, and C. Darrell Jennings

Subjects

Adult, Male, congenital, hereditary, and neonatal diseases and abnormalities, Myeloid, Adolescent, Biology, MLH1, medicine.disease_cause, DNA Mismatch Repair, Recurrence, hemic and lymphatic diseases, medicine, Humans, Child, Promoter Regions, Genetic, neoplasms, Molecular Biology, Adaptor Proteins, Signal Transducing, Aged, Aged, 80 and over, Mutation, Myeloid leukemia, Cancer, Infant, Nuclear Proteins, Cell Biology, DNA Methylation, Middle Aged, medicine.disease, digestive system diseases, Neoplasm Proteins, Leukemia, Leukemia, Myeloid, Acute, medicine.anatomical_structure, MutS Homolog 2 Protein, MSH2, Child, Preschool, Cancer research, DNA mismatch repair, Female, MutL Protein Homolog 1

Abstract

Acute myeloid leukemia (AML) is an aggressive hematological cancer. Despite therapeutic regimens that lead to complete remission, the vast majority of patients undergo relapse. The molecular mechanisms underlying AML development and relapse remain incompletely defined. To explore whether loss of DNA mismatch repair (MMR) function is involved in AML, we screened two key MMR genes, MSH2 and MLH1, for mutations and promoter hypermethylation in leukemia specimens from 53 AML patients and blood from 17 non-cancer controls. We show here that whereas no amino acid alteration or promoter hypermethylation was detected in all control samples, 18 AML patients exhibited either mutations in MMR genes or hypermethylation in the MLH1 promoter. In vitro functional MMR analysis revealed that almost all the mutations analyzed resulted in loss of MMR function. MMR defects were significantly more frequent in patients with refractory or relapsed AML compared with newly diagnosed patients. These observations suggest for the first time that the loss of MMR function is associated with refractory and relapsed AML and may contribute to disease pathogenesis.

Published

2008